QuickScreen Pro Multi Drug Screening Test Catalog # 9216T-25 Test Instructions

Transcription

1 QuickScreen Pro Multi Drug Screening Test Catalog # 9216T-25 Test Instructions Intended Use The QuickScreen Pro Multi Drug Screening Test is a rapid, self-timed, qualitative immunoassay for the detection of drugs of abuse in urine. The cutoff concentrations for the test are Barbiturates at 200 ng/ml, Benzodiazepines at 200 ng/ml, Methadone at 300 ng/ml, Amphetamine at 1000 ng/ml, Methamphetamine at 1000 ng/ml, Cocaine metabolite (Benzoylecgonine) at 300 ng/ml, THC metabolite (THCA) at 50 ng/ml, Opiates at 300 ng/ml and PCP at 25 ng/ml. This assay is intended for professional use. This test provides only a preliminary test result. A more specific alternate testing method must be used in order to obtain a confirmed analytical result. Gas chromatography/mass spectrometry (GC/MS) is the preferred confirmatory method. Other confirmation methods are available. Clinical consideration and professional judgment should be applied to any drug of abuse test result, particularly when preliminary positive results are observed. Summary & Explanation of the Test Barbiturates (BAR) are a large class of abused pharmaceuticals that are anxiolytic, sedative/hypnotic, anti-convulsant and anesthetic drugs. As CNS depressants, barbiturates affect excitatory and inhibitory synaptic neurotransmission. Ultra short-acting barbiturates used for anesthesia, such as Pentobarbital, depress excitatory neurotransmission to a greater extent than anti-convulsant barbiturates such as Phenobarbital. Barbiturates are rapidly and completely absorbed with nearly 100% bioavailability. Short-acting barbiturates are primarily excreted in urine as metabolites, while long-acting barbiturates are primarily excreted unchanged. Ratios of drugs to metabolites excreted vary, dependent upon duration of action. Benzodiazepines (BZD) are another large class of abused pharmaceuticals that are sedative/hypnotic and anti-anxiety drugs that produce calming effects; thus are often prescribed as tranquilizers. Frequently abused Benzodiazepines include Alprazolam (Xanax ), Diazepam (Valium ), Lorazepam (Ativan ), Triazolam (Halcion ), Chlordiazepoxide (Librium ), Flurazepam (Dalmane ) and Temazepam (Restoril ). A trend has been observed in recent years of abuse of these legitimate pharmaceuticals in conjunction with illicit controlled substances such as methadone and heroin. Benzodiazepines may be detected for up to 2 weeks in urine. Methadone (MTD) is a long-acting synthetic opiate agonist clinically available in the U.S. since Acting on the central nervous and cardiovascular systems, producing respiratory and circulatory depression, Methadone also produces meiosis and increases the tone of smooth muscle in the lower gastrointestinal tract while decreasing the amplitude of contractions. Amphetamine (AMP), Methamphetamine (MET 1000) and their metabolites are central nervous system stimulants whose pharmacological properties include alertness, wakefulness, increased energy, reduced hunger and an overall feeling of well being. Large doses and extended usage can result in higher 1

2 tolerance levels and physiological dependency. Both d and l forms of Amphetamine and the (+) form of Methamphetamine are controlled substances. Cocaine (COC) is an alkaloid present in coca leaves (Erythyroxine coca) whose pharmacological properties include alertness, wakefulness, increased energy and an overall feeling of euphoria. Cocaine has been used medicinally as a local anesthetic, however, its addictive properties have minimized its modern value as an anesthetic. Elimination of Cocaine is predominantly controlled by its biotransformation to Benzoylecgonine. Very low concentrations of Cocaine may be detected in urine during the initial several hours, but Benzoylecgonine persists in urine at detectable concentrations for 48 hours. 9 -Tetrahydrocannabinol (THC) is generally accepted as the principle active component in marijuana and hashish, although other cannabinoids contribute to their physiological activity. THC is rapidly absorbed by inhalation and through the gastrointestinal tract, and is almost completely metabolized. Its predominant metabolite, 11-Nor- 9 -Tetrahydrocannabinol-9-Carboxylic Acid, or THCA, is found in the plasma, feces and urine along with other compounds. Very low concentrations of THC may be detected in urine during the initial several hours after smoking, but THCA persists in urine at a detectable concentration for many days. Opiates (OPI) are addictive, pain-relieving narcotic drugs derived from the opium poppy (Papaver somniferum). An opiate is any natural or synthetic drug derived from this plant that has morphine-like pharmacological actions. Natural opiates include Morphine, Codeine and Thebaine. Synthetic opiates include Heroin, Hydrocodone and Levorphanol. Phencyclidine, also known as PCP or angel dust, is used primarily as a recreational drug for its hallucinogenic effects. Commonly taken orally, by inhalation, by sufflation or intravenously, it is well absorbed by all routes of administration, concentrating fastest in fatty tissues and the brain. Unchanged PCP is excreted in the urine in moderate amounts (10% of the dose). Terminal half-life varies considerably, ranging from 8 to 55 hours, though averaging 18. Effects of this drug are unpredictable and variable. Users may exhibit signs of euphoria, anxiety, relaxation, increased strength, time and space distortions, panic and hallucination. Urine based screening tests for drugs of abuse range from complex analytical procedures to simple immunoassay tests. The sensitivity and rapidity of immunoassays have made them the most accepted method of preliminary screening for drugs of abuse in urine. This allows the laboratory to eliminate the large number of negative specimens and focus on the smaller number of initially positive samples. Principle of the Procedure The QuickScreen Pro Multi-Drug Screening Test is a competitive immunoassay that is used to screen for the presence of drugs of abuse in urine. It is a chromatographic absorbent device in which drugs or drug metabolites in a sample compete with drug / protein conjugate immobilized on a porous membrane for a limited number of antibody /dye conjugate binding sites. The test device employs a unique combination of monoclonal and polyclonal antibodies to selectively identify drugs of abuse in urine with a high degree of confidence. The test device also contains a self-timer that indicates when test results are ready to be interpreted. In the procedure, the absorbent end of the test device is inserted into the urine sample. The urine is absorbed into the device by capillary action, mixes with the antibody / dye conjugate, and flows across the 2

3 pre-coated membrane. When sample drug levels are below the target cutoff (the detection sensitivity of the test), antibody / dye conjugate binds to the drug / protein conjugate immobilized in the Test Region (T) of the device. This produces a colored Test Band that, regardless of its intensity, indicates a negative result. When sample drug levels are at or above the target cutoff, the free drug in the sample binds to the antibody / dye conjugate, preventing the antibody / dye conjugate from binding to the drug / protein conjugate immobilized in the Test Region (T) of the device. This prevents the development of a distinct colored band, indicating a potentially positive sample. In either case, a colored Control Band is produced in the Control Region (C) by a non-specific antibodydye / conjugate reaction. This band serves as a built-in quality control device, demonstrating antibody recognition and reactivity as well as confirming that the test is complete. Reagents & Materials Supplied Self-Timed Test Devices (Cat. # 9216T); separate panels for each target drug contain: a. Monoclonal anti-drug antibody / colloidal gold conjugate in a protein matrix containing 0.1% sodium azide coated in the sample path b. Drug derivative / protein conjugate immobilized as a line in the Test Region (T) c. Goat anti-mouse antibody immobilized as a line in the Control Region (C) 2. Directional Insert (Cat. # 9216T-DI) 3. (Optional) Single Specimen Collection Kit (Cat. # 9501 or equivalent) or 4. (Optional) Split Specimen Collection Kit (Cat. # 9502 or equivalent) Warnings & Precautions 1. FOR IN VITRO DIAGNOSTIC USE ONLY. 2. For Professional use only. 3. Urine samples have the potential to be infectious. Follow Universal Precautions for proper handling and disposal methods. 4. Do not use this kit beyond its expiration date. 5. This method is established using urine only. No other fluid has been evaluated. 6. Do not reuse the Test Device. Storage & Handling Requirements Store at room temperature (15 28 C). Do not freeze. Refer to expiration date for stability. 3

4 Sample Collection & Preparation A fresh urine sample should be collected in one of the above-mentioned specimen collection kit or equivalent. Alternately, a clean, dry plastic or glass container, unused and without preservatives, may be used for specimen collection. Testing requires at least 1 / 2 -inch (50 60 ml) of urine in the sample container. If required by your procedure, aliquot a portion of urine into the split sample container for later confirmation of results. If not required, dispose of all but 1 / 2 -inch of urine and save the remainder for the QuickScreen test. Samples may be tested immediately or stored for up to 48 hours at 2 8 C. For longer storage, freeze samples at 20 C or below. Assay Procedure Preparation 1. Confirm that samples and test components are at room temperature ( C) before testing. 2. Do not break the seal on the foil pouch until you are ready to perform the test. Testing 1. Open the foil pouch at the notch and remove the test device. Take care not to touch the exposed membranes. 2. Insert the reactive end of the test device into the urine sample. Make sure that the urine level is not above the MAX URINE LEVEL printed on the front of the device. 3. Leave the test device in the sample cup until you are ready to read the test results. 4

5 When to Read Test Results Using the Timer When the RESULT READY window is completely filled with red color, or is almost completely covered with red color that reaches the top of the window, the test results are ready to interpret. When red color becomes clearly visible at the bottom of the RESULT EXPIRED window, test results should no longer be interpreted and should not be considered as conclusive. Interpretation of Test Results Negative Test Results for All Drugs Tested Negative A negative result is indicated when two (2) colored bands appear, one in the Control Region (C) and one in the Test Region (T), before any red color appears at the bottom of the RESULT EX- PIRED window. This result indicates that the target drug is not present or its concentration is below the detection sensitivity of the test panel. Some negative results may appear in as little as 1 minute, and can be safely interpreted as soon as 2 colored bands are visible. 5

6 Positive Test Results for Cocaine and Methadone Positive A positive result is indicated when only one (1) colored band appears in the Control Region (C) and no band appears in the Test Region (T), after a red spot appears in the RESULT READY window. This result indicates that the target drug concentration is at or above the detection sensitivity of the panel. More than one panel may be positive. Potentially positive results can only be reported when a red spot appears in the timer s RE- SULT READY window, and before any red color appears at the bottom of the timer s RESULT EXPIRED window. Invalid A test must be considered invalid if, after a red spot appears in the RESULT READY window, no bands appear or if a band appears in the Test Region without a Control Band. The presence of a Control Band is necessary to confirm assay performance. Quality Control Invalid Test Results for THC and Opiates An internal procedural control line has been incorporated into the test device to help ensure proper kit performance and reliability. However, the use of external controls is recommended. Positive and negative controls within 25% of the cutoff concentration should produce the expected results. For positive controls, only one (1) colored band will appear in the Control Region (C), and no band will appear in the Test Region (T). For negative controls, two (2) colored bands will appear, one in the Control Region (C) and one in the Test Region (T). Limitations of the Procedure 1. It is possible that substances and factors not described in this directional insert may interfere with the test, causing false results (e.g. technical or procedural error). 2. This test has been developed for testing urine samples only. Its performance using other specimens has not been substantiated. 6

7 3. Adulterated urine samples may produce erroneous results. Strong oxidizing agents such as bleach (hypochlorite) can oxidize drug analytes. If a sample is suspected of being adulterated, a new sample must be obtained. 4. All preliminary positive results must be confirmed by another method. Gas chromatography/mass spectrometry (GC/MS) is the method of choice to confirm the presence and concentration of a drug in urine. 5. This test is a qualitative screening assay. It is not designed to determine the quantitative concentration of target drugs or the level of intoxication. 6. Because QuickScreen is a competitive assay no prozone effect is present. 7. Occasionally, samples containing target drugs below the target drug s cutoff sensitivity for the test may produce a positive result. 8. Point-of-care testing data is not currently available. Performance Characteristics Cross-Contamination The QuickScreen Pro Multi Drug Screening Test was tested to ensure that the individual test panels, when assembled in the multi-panel device, had no effect on expected results. Urine samples were selected which had no target drugs present. These samples were aliquoted and spiked with target drugs / metabolites in varied combinations at 125% of the target drug cutoffs. All samples were coded and assayed in a blind study by 2 laboratory technicians using 3 lots of Quick- Screen. The QuickScreen Pro Multi Drug Test gave 100% correct results for all samples tested. No false results due to crossover or interaction between individual test panels were observed. Cross-Contamination Study Results; Expected vs. Observed Sample / Panel BAR BZD MTD AMP MET COC THC OPI PCP ( ) for all drugs ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) (+) for BAR only (+)/(+) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) (+) for BZD only ( )/( ) (+)/(+) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) (+) for MTD only ( )/( ) ( )/( ) (+)/(+) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) (+) for all drugs except BAR ( )/( ) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+) for all drugs except BZD (+)/(+) ( )/( ) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+) for all drugs except MTD (+)/(+) (+)/(+) ( )/( ) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+) for BAR & BZD only (+)/(+) (+)/(+) ( )/( ) ( )/( ) (+)/(+) ( )/( ) ( )/( ) ( )/( ) ( )/( ) (+) for BZD & MTD only ( )/( ) (+)/(+) (+)/(+) ( )/( ) (+)/(+) ( )/( ) ( )/( ) ( )/( ) ( )/( ) (+) for BAR & MTD only (+)/(+) ( )/( ) (+)/(+) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) (+) for BAR, BZD & MTD only (+)/(+) (+)/(+) (+)/(+) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) ( )/( ) (+) for all drugs (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) (+)/(+) Note: Remaining performance characteristics were determined using the strip versions of the individual test panels. 7

8 Kit Comparison The performance of the QuickScreen Pro Multi Drug Test was evaluated on clinical urine samples and compared with a commercially available assay at the stated cutoff concentrations for relative sensitivity and specificity and for overall agreement. Results from in-house studies and combined studies of 2 independent clinical laboratories are reported, comparing QuickScreen results with the EMIT instrument-based immunoassay. In-House Study Data - % Agreement Target Drug BAR BZD MTD AMP MET COC OPI THC PCP n = Relative Sensitivity >99 >99 > >99 >99 >99 99 Relative Specificity >99 88 >99 >99 >99 96 >99 >99 99 Overall Agreement >99 94 > >99 >99 >99 [1] [2] Clinical Study Data - % Agreement Target Drug BAR BZD MTD AMP MET COC THC OPI PCP n = Relative Sensitivity >99 > >99 98 >99 95 Relative Specificity [1] >99 >99 > [2] 99 >99 99 Overall Agreement >98 > samples at 324 and 336 ng/ml (8% and 12% above cutoff, respectively) gave negative results in the Methadone Clinical Study. 5 discrepant results were observed in the Cocaine Clinical Study; the samples were from 3 to 10% below the assay cutoff concentration (271 to 293 ng/ml) and subsequently tested positive by GC/MS. Precision Eight urine pools ranging in concentration from 0 to 200% of cutoff were assayed twice a day for 20 days. Results were interpreted individually by 2 technicians. The precision of the Quick- Screen Pro Test was determined to be >95% for all assays. Cross-Reactive Substances The following compounds were spiked into normal human urine and tested for cross-reactivity with the QuickScreen Pro Multi Drug Screening Test. The results (in µg/ml) are expressed as that amount of compound capable of giving a result equivalent to the target drug at its cutoff concentration. Except as noted, a blank space indicates that no cross-reactivity was observed when the compound was tested to 100 µg/ml. (See chart next page). 8

9 Compound BAR BZD MTD AMP MET COC THC OPI PCP Amobarbital 0.15 Aprobarbital 0.05 Barbital Butabarbital Pentobarbital Butalbital 0.3 Butethal ,5-Diallylbarbituric Acid 0.1 Phenobarbital Secobarbital 0.2 (±)-Thiopental 9.5 Alprazolam [A] Clonazepam 0.5 Bromazepam 0.6 Chlordiazepoxide 0.3 Desmethyldiazepam 0.75 Diazepam Flunitrazepam 0.4 Flurazepam Medazepam Prazepam 1.0 (±)-Lorazepam Triazolam [B] 0.5 Lormetazepam 0.4 Nitrazepam Oxazepam 0.2 Temazepam 0.25 ( )-α-acetylmethadol (LAAM) 1 ( )-α-methadol 0.8 (±)-Methadone 0.3 d-amphetamine 1 dl-amphetamine 3-Hydroxytyramine 10 l-amphetamine (R)-(+)-α-Phenylethylamine 100 Mephentermine (±)-3,4-Methylenedioxyamphetamine 4.5 (±)-α-phenylethylamine β- 10 Phenylethylamine Tyramine 12.5 ( )-Deoxyephedrine Nylidrin 10 (+)-Methamphetamine 1 (±)-3,4-Methylenedioxymethamphetamine 5 Benzoylecgonine Cocaine 0.3 Metoclopramide 25 Procaine Pyrilamine Hydroxy- 9 -THC [C] 1 11-Nor- 8 -THC-9-Carboxylic Acid [C] Nor- 9 -THC-9-Carboxylic Acid [C] Tetrahydrocannabinol Tetrahydrocannabinol 0.05 Codeine Heroin [B] 0.3 Dextromethorphan 50 Ethylmorphine [B] 0.35 Hydrocodone Hydromorphone 0.4 Levorphanol Nalorphine Norcodeine 0.5 Morphine Morphine-3-β-D-Glucuronide 0.3 Naloxone 0.4 9

10 Naltrexone 5 Normorphine [B] 10 Oxycodone Thebaine 0.6 EDDP (Primary Methadone Metabolite) 25 Phencyclidine [A] [B] [C] A blank space indicates that no cross-reactivity was observed when the compound was tested to 25 µg/ml. A blank space indicates that no cross-reactivity was observed when the compound was tested to 10 µg/ml. A blank space indicates that no cross-reactivity was observed when the compound was tested to 5 µg/ml. Interfering Substances The following compounds were spiked into normal human urine and tested for interference with the QuickScreen Pro Multi Drug Screening Test. The compounds were tested to 100 µg/ml, except as noted, with no interference observed. Acetaminophen Acetoacetic Acid Acetone N-Acetylprocainamide Acetylsalicylic Acid (Aspirin) Albumin Alphenal Amantadine (+)-Amethopterin Amikacin dl-aminoglutethimide Aminopyrine Amitriptyline Amoxicillin Ampicillin Apomorphine ( )-Arterenol l-ascorbic Acid (Vitamin C) Aspartame d-aspartic Acid dl-aspartic Acid l-aspartic Acid Atropine Barbituric Acid Benzoic Acid Benzphetamine Benztropine Methane Sulfonate Bilirubin Bromocriptine Mesylate (+)-Brompheniramine Caffeine Cannabidiol Cannabinol Carbamazepine Cephalexin Chloramphenicol Chloroquine (+)-Chlorpheniramine (±)-Chlorpheniramine Chlorpromazine Chlorpropamide Chlorprothixene Cimetidine Clemastine Clomipramine Clonidine ( )-Cotinine Creatinine Cyclizine Cyclobenzaprine Cyclosporin A Cyproheptadine Desipramine Diflunisal Digoxin 4-Dimethylaminoantipyrine Diphenhydramine Diphenoxylate 5,5-Diphenylhydantoin Disopyramide Doxepin Doxylamine (+)-ψ-ephedrine ( )-ψ-ephedrine (+)-Ephedrine (±)- Ephedrine ( )-Ephedrine (±)-Epinephrine ( )-Epinephrine Erythromycin Estriol Estrone-3- Sulfate Ethanol Ethosuximide Ethyl-p-Aminobenzoate Ethylenediaminetetraacetic Acid EMDP (Secondary Methadone Metabolite) Fenfluramine Fenoprofen Fentanyl [D] Furosemide Gentamicin Gentisic Acid Glucose dl-glutethimide Griseofulvin Guaiacol Glyceryl Ester Hexobarbital Human Hemoglobin Hydrochlorothiazide dl-β-hydroxybutyric Acid o-hydroxyhippuric Acid 5- Hydroxyindole-3-Acetic Acid 5-Hydroxyindole-2-Carboxylic Acid Hydroxyzine Ibuprofen Imipramine Indole-3-Acetic Acid Indole-3-Butyric Acid Indomethacin (+)-Isoproterenol (±)- Isoproterenol ( )-Isoproterenol Isoxsuprine Kanamycin Ketamine Ketoprofen Labetalol Lidocaine Lithium Carbonate Lysergic Acid Diethylamide (LSD) [E] Melanin Meperidine Meprobamate Mescaline dl-metanephrine Methaqualone (S)-6-Methoxy-α-Methyl-2-Naphthaleneacetic Acid 2-Methyl-3-(3,4-Dihydroxyphenyl)-dl-Alanine 2-Methyl-3-(3,4-Dihydroxyphenyl)-l-Alanine Methylphenidate Methyprylon (±)-Metoprolol Nafcillin Naphazoline α-naphthaleneacetic Acid β-naphthaleneacetic Acid Naproxen Netilmicin Niacinamide Nialamide Nicotinic Acid Nifedipine Nomifensine Nordoxepin [D] Norethindrone Nortriptyline Noscapine Orphenadrine Oxalic Acid Oxymetazoline Papaverine Penicillin G Pentazocine Phenelzine Pheniramine Phenothiazine Phentermine Phenylacetone l-phenylalanine Phenylbutazone trans-2- Phenylcyclopropylamine l-phenylephrine (±)-Phenylpropanolamine Piroxicam Potassium Chloride Prednisolone Primidone Procainamide Prochlorperazine Promazine Promethazine (+)- Propoxyphene 2-Propyl-pentanoic Acid Protriptyline Quinidine Quinine Ranitidine Riboflavin Salicylic Acid ( )-Scopolamine Sodium Chloride Sulindac Terbutaline Tetracycline Tetraethylthiuram Disulfide (Antabuse) Tetrahydrozoline Theophylline Thioridazine cis-thiothixene Tobramycin Triamterene Trifluoperazine Triflupromazine dl-trihexyphenidyl Trimethobenzamide Trimethoprim Trimipramine Triprolidine Urea Uric Acid Vancomycin (±)- Verapamil Zomepirac [D] No interference was observed when the compound was tested to 10 µg/ml. [E] No interference was observed when the compound was tested to 2.5 µg/ml. 10

11 Endogenous Conditions Urine conditions of ph, ranging from 4.5 to 8.5, and specific gravity, ranging from to 1.040, were tested in normal human urine with the QuickScreen Pro test and found to have no effect on expected results. Bibliography & Suggested References 1. Federal Register, Department of Health and Human Services, Mandatory Guidelines for Federal Workplace Drug Testing Programs (1988) 2. Urine Testing for Drugs of Abuse, NIDA Research Monograph 73, (1986) 3. Dasgupta A., Saldana S., Kinnaman G., Smith M., Johansen K., Clinical Chemistry 39: (1993) 4. Liu R.H., Goldberger B.A., Handbook of Workplace Drug Testing, AACC Press (1995) 5. Jeffcoat A.R., et al, Drug Metabolism and Disposition, 17-2 (1989) 6. Inaba T., Journal of Canadian Physiology and Pharmacology, 67: (1989) 7. Karch S.B., Drug Abuse Handbook, CRC Press (1998) QuickScreen Pro Multi Drug Screening Test Catalog # 9216T-25 FOR IN VITRO DIAGNOSTIC USE ONLY For Ordering Information Contact: Phamatech, Inc Padgett Street, Suite 101 San Diego, CA Tel: (858) Fax: (858) Website: T-DI, Doc. # , Rev. A, Eff. 12/06/00 11